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Title Page

Title Real-World Outcome of Rheumatoid Arthritis Patients in Korea on Adalimumab (ROCKA Study)

Protocol Version Identifier Amendment 01, 26 Dec 2017Date of Last Version ofProtocol 26 Dec 2017

EU PAS Register Number Not registered (Non-PASS PMOS)Active Substance Not applicable (Non-PASS PMOS)Medicinal Product Not applicable (Non-PASS PMOS)Product Reference Not applicable (Non-PASS PMOS)Procedure Number Not applicable (Non-PASS PMOS)Marketing Authorization Holder(s)

AbbVie Limited

Joint PASS Not applicable (Non-PASS PMOS)Research Question and Objectives

The overall strategic objective of this non-interventional, observational study is to assess the effect of Adalimumab on health-related quality of life and work productivity in patients with Rheumatoid Arthritis (RA) in Korea.

Country(ies) of Study KoreaAuthor

This study will be conducted in compliance with this protocol. Confidential Information

No use or disclosure outside AbbVie is permitted without prior written authorization from AbbVie.

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Marketing Authorization Holder(s)

Marketing Authorization Holder(s) AbbVie Ltd

MAH Contact Person Not applicable (Non-PASS PMOS)

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1.0 Table of Contents

1.0 Table of Contents .................................................................. 3

2.0 Abbreviations ........................................................................ 6

3.0 Responsible Parties ............................................................... 7

4.0 Abstract ................................................................................. 9

5.0 Amendments and Updates .................................................. 14

6.0 Milestones ............................................................................ 14 7.0 Rationale and Background ................................................. 14

8.0 Research Question and Objectives ..................................... 15

9.0 Research Methods ............................................................... 16

Study Design ........................................................................................ 16 9.1 Schedule of Events ............................................................................... 18 9.1.1

Setting .................................................................................................. 18 9.2 Inclusion Criteria: ................................................................................. 19 9.2.1 Exclusion Criteria: ................................................................................ 19 9.2.2 Investigator Selection Criteria .............................................................. 20 9.2.3 Study Procedures .................................................................................. 20 9.2.4

9.2.4.1 Informed Consent ................................................................................. 20

9.2.4.2 Patient Assignment ............................................................................... 20 9.2.4.3 Investigator Recruitment ...................................................................... 21

9.2.4.4 Study site monitoring ........................................................................... 21

9.2.4.5 Patient Selection ................................................................................... 21

9.2.4.6 Data Collection..................................................................................... 22

9.2.4.7 Study Documents ................................................................................. 22

Adverse Events..................................................................................... 25 9.2.5 Variables .............................................................................................. 25 9.3 Data Sources ........................................................................................ 25 9.4 Study Size ............................................................................................ 26 9.5 Data Management and Storage Process................................................. 26 9.6

Data Management ................................................................................ 26 9.6.1 Storage Process .................................................................................... 27 9.6.2

Data Analysis ....................................................................................... 27 9.7

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Statistical and Analytic plans ................................................................ 27 9.7.1 Analyzable population .......................................................................... 27 9.7.2 Planned Methods of Statistical Analysis ............................................... 28 9.7.3 Primary Endpoint Analysis ................................................................... 28 9.7.4 Secondary Endpoint Analysis ............................................................... 28 9.7.5 Additional Secondary Endpoint Analysis .............................................. 29 9.7.6 Safety Analysis..................................................................................... 29 9.7.7 Additional Analysis .............................................................................. 30 9.7.8 Missing Data ........................................................................................ 30 9.7.9

Interim Analysis ................................................................................... 30 9.7.10 Quality Control..................................................................................... 30 9.8

Ethics and Quality ................................................................................ 30 9.8.1 Quality Assurance ................................................................................ 30 9.8.2

Limitations of the Research Methods .................................................... 31 9.9 Other Aspects ....................................................................................... 31 9.10

Note To File ......................................................................................... 31 9.10.1 Training Log ........................................................................................ 32 9.10.2 Visitor Log ........................................................................................... 32 9.10.3 Responsibilities of the Principal Investigator ........................................ 32 9.10.4 End of Trial .......................................................................................... 32 9.10.5

10.0 Protection of Human Subjects ............................................ 32

11.0 Management and Reporting of Complaints ....................... 33 Medical Complaints ............................................................................. 33 11.1

Adverse Event Definition and Serious Adverse Event Categories ......... 33 11.1.1 Severity ................................................................................................ 35 11.1.2 Relationship to Pharmaceutical Product ................................................ 35 11.1.3 Serious Adverse Event Collection Period.............................................. 36 11.1.4 Serious Adverse Event Reporting ......................................................... 36 11.1.5 Pregnancy Reporting ............................................................................ 36 11.1.6 Malignancy Reporting .......................................................................... 36 11.1.7

Product Complaint ................................................................................ 37 11.2 Definition ............................................................................................. 37 11.2.1 Reporting ............................................................................................. 37 11.2.2

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12.0 Ethical and Legal Consideration ........................................ 38

13.0 Confidentiality ..................................................................... 39

Patient confidentiality ........................................................................... 39 13.1 Data confidentiality .............................................................................. 39 13.2

14.0 Study administration ........................................................... 39

15.0 Investigators compliance ..................................................... 40

16.0 Risks ..................................................................................... 40

17.0 Discontinuation or Drop-out ............................................... 40

18.0 Quality control and audit .................................................... 41

19.0 Communication of findings................................................. 41 20.0 References ............................................................................ 41

21.0 Appedndices......................................................................... 44

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2.0 Abbreviations

ACR American College of Rheumatology AE Adverse Events AESI Adverse Event of Special Interest ANOVA Analysis of Variance CRF Case Report Form CRP C-Reactive Protein CTCAE Common Terminology Criteria for Adverse Events DAS28 Disease Activity Score in 28 Joints EQ-5D-3L EuroQol 5 dimension, 3 level quality of life questionnaire ESR Erythrocyte Sedimentation Rate EULAR The European League Against Rheumatism GP General Practitioner HAQ DI Health Assessment Questionnaire Disability Index HCRU Healthcare Resource Utilization ICF Informed Consent Form ICH-GCP International Conference on Harmonization of Good Clinical

Practice NRS Numeric Rating Scale PGIC Patient Global Impression of Change PHI Protected Health Information PRO Patient-Reported Outcome QC Quality Check QoL Quality of Life RA Rheumatoid Arthritis SAP Statistical Analysis Plan SF-36 Short Form 36-Item Health Survey SOC System Organ Class SOP Standard Operating Procedure TNF Tumor Necrosis Factor VAS Visual Analogue Scale WPAI Work Productivity and Activity Impairment

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3.0 Responsible Parties

Study-Designated Physician/Sponsor:

Statistics Manager/ CRO(S):

Principal Investigator: Investigator information is on file at AbbVie

Sponsor:

Clinical Project Manager:

Emergency ContactsSafety Review Team

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PROTOCOL SIGNATURES Investigator Signature: I have read and agree to the Protocol Number 11006, “Real-World Outcome of Rheumatoid Arthritis Patients in Korea on Adalimumab (ROCKA Study)”. I am aware of my responsibilities as an investigator under the guidelines of Good Clinical Practices, local laws and regulations (as applicable) and the study protocol. I agree to conduct the study according to these laws and guidelines and to appropriately direct and assist the staff under my control, who will be involved in the study. Principal (Site) Investigator: Name (typed or printed):

Institution and Address:

Telephone Number:

Signature: Date: (Day/ Month /Year) Full investigational site contact details, including telephone numbers, will be documented in the Study Master File.

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4.0 Abstract

Title: Real-World Outcome of Rheumatoid Arthritis Patients in Korea on adalimumab (ROCKA Study). Rationale and Background: Given the requirement to keep a balance between effectiveness and cost containment to ensure that the available health resources are used in a cost-effective manner, there is an increasing demand for real-world evidence (RWE) from policy makers, regulators, providers and payers in the region to optimize spending and patient outcomes. So far, there are no data available regarding adalimumab’s impact on patients’ quality of life (QoL) and healthcare resource utilization (HCRU) in a realistic study design in Korea. The goal of this study is to determine the QoL, HCRU and costs of the patients care in subjects with RA who are treated with adalimumab in Korea. Results from study on the effect of adalimumab on Work Productivity and Activity Impairment (WPAI) scores and other Patient-Reported Outcomes (PROs) will be of interest to a variety of stakeholders in the healthcare system including patients, healthcare practitioners and payers in Korea. Research Question and Objectives: The objective of this non-interventional, observational study is to assess the effect of adalimumab on health-related QoL and work productivity in patients with Rheumatoid Arthritis (RA) in Korea. Specifically, to achieve the above objective the following concrete steps will be taken:

1. Recruit investigators who are willing and able to recruit and follow new adalimumab users for 6 months follow-up

2. Collect the patients’ clinical profile, patient-reported QoL, functioning, work productivity, treatment satisfaction and HCRU of RA patients at adalimumab initiation

3. Follow the patients initiating adalimumab for 24 weeks and identify the changes in clinical, economic, and PROs associated with adalimumab

Study Design: The study is designed as a prospective, observational study to assess the effect of adalimumab on health-related QoL and work productivity in patients with RA in Korea. Note: This study is non-interventional and the subjects/investigators will follow the current clinical practice in each site and also the routine clinical follow up as determine by the treating physician.

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RA patients, for whom adalimumab treatment has already been decided, will be recruited from within the clinical settings of each rheumatologist participating in the study. Approximately 89 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea. To assess health and disability outcomes, the Health Assessment Questionnaire Disability Index (HAQ DI) will be assessed at baseline, Week 12 and Week 24 after treatment initiation with adalimumab. In addition, other PROs of work activity and well-being, including the WPAI, EuroQol 5 dimension (EQ-5D), and Short Form 36-Item Health Survey (SF-36), will also be assessed. In addition, the health care resource utilization will be collected. This includes surgical procedures, hospitalizations, bed days in hospital, physician consultations etc. Costs will be assigned based on the health care resource utilization using standardized costs for participating country. Population: Subjects will be males and/or females who are attending a routine clinical visit and meet all of the inclusion criteria and none of the exclusion criteria. Approximately 89 patients diagnosed with RA will be recruited. Inclusion Criteria: Patients meeting all of the following inclusion criteria at baseline will be included:

1. Subject has a diagnosis of RA as defined by the 1987 revised American College of Rheumatology (ACR) classification criteria and/or the ACR/the European League against Rheumatism (EULAR) 2010 classification criteria (any duration since diagnosis).

2. Male or female subject ≥18 years of age (local definition according to adalimumab label) who is in compliance with eligibility for adalimumab based on the local label.

3. Patients with moderate to severe RA defined as Disease Activity Score in 28 Joints (DAS28) (ESR) or DAS28 (CRP) >3.2

4. Biologically treatment naïve and initiated adalimumab at baseline visit 5. Availability of clinical data of the previous 12 weeks prior to baseline 6. Ability to self-complete patient questionnaires 7. Subject must be able and willing to provide written informed consent and

comply with the requirements of this study protocol. Exclusion Criteria: Patients meeting any of the following exclusion criteria at baseline will be excluded:

1. Patients who are pregnant or breast feeding at enrolment or wish to become pregnant in the next 24 weeks.

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2. Participation in any RA-related clinical trial at the time of enrolment, at baseline or at any point during the past 24 weeks prior to baseline

3. Patients, who in the clinician’s view, may not be able to accurately report their QoL or prior resource utilization

4. Patients, who in the clinician’s view, may not be able to adhere to adalimumab therapy over 24 weeks.

Variables: Primary Variable

Change in HAQ DI score at weeks 12 and weeks 24 weeks from the baseline

Secondary Variable Change in other PROs (SF-36 domain scales, EQ-5D Index, Work Productivity

and Activity Impairment Questionnaire [WPAI]) from baseline to weeks 12 and 24

Number and percent of patients achieving a clinically meaningful improvement on the HAQ DI, from baseline to weeks 12 and 24

Healthcare Resource Utilization (HCRU) at baseline, 12 and 24 weeks

Additional Secondary Variable Change in HAQ DI score from baseline to 24 weeks Changes in the disease severity and PROs from baseline to 24 weeks

Exploratory Variable Change in patient satisfaction questions from baseline to weeks 12 and 24

Data Sources: Case Report Forms (CRFs) and patient questionnaires. Collection of data includes but not limited to subject demographics, clinical history, comorbidities, spontaneous adverse events, and concomitant medications. The following questionnaires will be utilized to collect data directly from participating subjects:

EQ-5D SF-36 HAQ DI WPAI HCRU Patient Global Impression of Change (PGIC) Patient Treatment Satisfaction Questions

Study Size: Approximately 89 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea. The sample size was calculated by assuming an alpha of 0.05 and a power of 0.80 in a one-sided test,

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resulting in 36 subjects required to recognize a statistically significant improvement in HAQ DI (-0.21). Then, given the importance of other secondary endpoints, an improvement of 9.9±25 hours of work time lost requires 40 subjects. However, since it is expected that approximately half the study population may no longer be working due to their age, we assume a 50% employment rate in the study population and a drop-out rate of 10%, eventually approximately 89 patients will be required to achieve the required number of respondents. Data Analysis: Primary Endpoint Analysis Change in HAQ DI score at 24 weeks after the initiation of adalimumab (observed population). This change will be summarized as the mean and 95% confidence interval and will be tested with a paired t-test.

Secondary Endpoint Analysis Change in other PROs (SF-36 domain scales, EQ-5D Index, WPAI total lost

productivity) at weeks 12 and 24 after the initiation of adalimumab (observed population). These changes will be summarized as the means and 95% confidence intervals and will be tested with paired t-tests.

Number and percent of patients achieving a clinically meaningful improvement on the HAQ DI, as defined by a -0.22 point improvement or greater, at weeks 12 and 24 after the initiation of adalimumab (observed population).

Additional Secondary Endpoint Analysis Change in HAQ DI score at 24 weeks after the initiation of adalimumab

(observed population), compared with those patients not continuing on adalimumab (non-observeds). The mean changes in these two groups will be compared using an independent t-test.

HCRU will be described using number and percentage within each category (number of consultations, number of procedures received, number of surgeries, number of hospitalizations and length of stay, number of concomitant medications)

Associations between disease severity and PROs Associations between change in disease severity and change in PROs

Exploratory endpoint Change in patient satisfaction questions at weeks 12 and 24 after the initiation

of adalimumab (observed population). These changes will be summarized as number and percentage of each response and compared with Kruskal–Wallis test. Satisfaction will also be dichotomized and analyzed over time with

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Cochrane-Armitage test for trends. Milestones: Start of Data Collection : 19 Oct, 2015 End of Data Collection : 28 Feb, 2018 Study Progress Report : Not applicable Interim Report : Not applicable Registration in the EU PASS Register : Not Applicable Final Report of Study Results : 31 Aug, 2018

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5.0 Amendments and Updates

Number Date Section of Study Protocol

Amendment or Update Reason

1 26 Dec 2017 - Sample size - Milestones

Amendment

Change of sample size and

milestones (See Appendix L for details)

6.0 Milestones

Major study milestones and their planned dates are as follows:

Start of Data Collection (FPFV): 19 October 2015 End of Data Collection: 28 February 2018 Study Progress Report: Not Applicable Interim Report: Not Applicable Registration in the EU PAS register: Not Applicable Final Report of Study Results: 31 August 2018

7.0 Rationale and Background

Disability has been defined as impairments, activity limitations and participation restrictions due to personal and environmental factors (1). The concept of disability is one where a physical health condition or disease is evaluated in terms of its impact, difficulties, or limitations on a range of tasks, activities, or roles that are considered typical of everyday life. Examples of affected activities include basic aspects of daily living such as eating, bathing, dressing, household chores and meal preparation, or participation in society, or participation in work. For public health purposes disability is becoming increasingly important as an outcome measure. Despite this, no data, within our knowledge, on the effectiveness of adalimumab on health-related QoL and work productivity in patients with Rheumatoid Arthritis (RA) in Korea.

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Results from study of effect of adalimumab on Work Productivity and Activity Impairment (WPAI) scores and other Patient-Reported Outcomes (PROs) of work activity and well-being will be of interest to a variety of stakeholders in the healthcare system including patients, healthcare practitioners and payers in Korea. Reimbursement in Korea is strongly influenced by local “real -world” evidence of the intervention’s effects on outcomes and economic endpoints. Therefore, having the economic and health outcomes “real world evidence” (RWE) for the use of Humira in moderate RA patients from Korea will be valuable to support the reimbursement / pricing maintenance and expansion in Korea. In Korea, Humira is reimbursed for both moderate and severe RA patients. However, the recent policy change in Korea indicated that the paradigm of using the ICER as the only value metric has been recently shifting toward considering other criteria such as patient reported outcomes, equity, innovation, and affordability. For example, the Korean government is in discussion with industry and academics to incorporate multi-criteria decision analysis (MCDA) such as including patient reported outcome into HTA for new medical technologies and post launch product price management. In this regard, generating the RWE is critical for the price re-negotiation and protection with the national payer, under current reimbursement and pricing policies in South Korea. The objective of this non-interventional, observational study is to assess the effect of adalimumab on health-related QoL, work productivity, and healthcare resource utilization (HCRU) in patients with RA in Korea. The Humira’s efficacy and patient’s outcomes data from this study could be used to mitigate the tapering issues of biologics. The patients’ work-productivity data aligned with global comparison could be used to keep the current co-payment ratio, 10% of patients. And aligned with T2T and fit for work data, we can pursue to expand the importance of early treatment of RA.

8.0 Research Question and Objectives

The objective of this study is to assess the effect of adalimumab on health and disability outcomes in patients with the immune-mediated inflammatory diseases of rheumatoid arthritis. The effect of adalimumab on health and disability outcomes in these patients will be assessed by the primary outcome measure which is the change in Health Assessment Questionnaire Disability Index (HAQ DI) score at 24 weeks after the initiation of adalimumab. The HAQ DI is selected as the primary point as it is commonly used to assess improvements in physical function in RA clinical trials and recommended by the US Food and Drug Administration (FDA) guidance on RA treatment development (3, 4).

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In addition, the HAQ-DI has been utilized as a predictor variable in investigations of productivity (5). The HAQ-DI has been demonstrated to be significantly correlated with work-related measures such as work capacity, household work performance, work task performance, and work disability (6-9). In addition, the effect of adalimumab will also be assessed by the secondary outcome measures which are changes to the WPAI, EuroQol 5 dimension (EQ-5D) score, and Short Form 36-Item Health Survey (SF-36) domain scores at 12 and 24 weeks after the initiation of adalimumab in RA.

9.0 Research Methods

Study Design 9.1

This study is designed as a prospective, observational study to assess the effect of adalimumab on health-related QoL and work productivity in patients with RA in Korea in clinical practice. Note: This study is non-interventional and the subjects/investigators will follow the current clinical practice in each site and also the routine clinical follow up as determine by the treating physician. RA patients will be recruited from within the clinical settings of each rheumatologist participating in the study. Approximately 89 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea. To assess health and disability outcomes, the HAQ DI will be assessed at baseline, Week 12 and Week 24 after treatment initiation with adalimumab. In addition, other PROs of work activity and well-being, including the WPAI, EQ-5D, and SF-36, will also be assessed. The patients identified by the recruiting investigators (specialty dependent on country/region; e.g. rheumatologist, internists, general practitioners, etc.) based on the study selection criteria will complete a set of patient questionnaires on QoL, functioning, work productivity, treatment satisfaction, impression of change and HCRU. Data will be captured at baseline (D0), Week 12 and Week 24. The HCRU will also be collected. This includes surgical procedures, hospitalizations, bed days in hospital, physician consultations etc. Costs will be assigned based on the HCRU using standardized costs for each participating countries.

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Subjects may discontinue adalimumab treatment at any time during study participation. Subjects that end study participation early will have a Termination Visit. All subjects will have a follow-up phone call approximately 70 days after the last administration of adalimumab to obtain information on any new or ongoing AEs. This protocol requires all SAEs and AESIs as outlined in protocol section 11.0 to be actively solicited. The safety profile of adalimumab which has over 3.5 million patient years of post-marketing exposure is stable and well established; non-serious events will not be actively solicited as these events are not likely to contribute to the further understanding of the safety profile of the product. Any non-serious AEs will be collected as spontaneous reports if AbbVie is notified. As this is a postmarketing observational study, Abbvie is NOT involved in the product supply since the drug is being used according to the approved market label and is to be prescribed by the physician under usual and customary practice of physician prescription. This study is non-interventional and the subjects/investigator will follow the current clinical practice in each site. Not additional task will be required other than current practice to keep the data as “real world data collect. Primary EndpointChange in HAQ DI score at 24 weeks after the initiation of adalimumab(observed population). This change will be summarized as the mean and 95% confidence interval and will be tested with a paired t-test. Secondary Endpoint Analysis

Number and percent of patients achieving a clinically meaningful improvement on the HAQ DI, as defined by a -0.22 point improvement or greater, at weeks 12 and 24 after the initiation of adalimumab (observed population).

Additional Secondary Endpoint Analysis Change in HAQ DI score at 24 weeks after the initiation of adalimumab (observed

population), compared with those patients not continuing on adalimumab (non-observeds). The mean changes in these two groups will be compared using an independent t-test.

Healthcare resource utilization will be described using number and percentage within each category (number of consultations, number of procedures received, number of surgeries, number of hospitalizations and length of stay, number of concomitant medications)

Associations between disease severity and PROs Associations between change in disease severity and change in PROs

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Change in other patient reported outcomes (SF-36 domain scales, EQ-5D Index, WPAI total lost productivity) at weeks 12 and 24 after the initiation of adalimumab (observed population). These changes will be summarized as the means and 95% confidence intervals and will be tested with paired t-tests.

Change in patient satisfaction questions at weeks 12 and 24 after the initiation of adalimumab (observed population). These changes will be summarized as number and percentage of each response and compared with Kruskal–Wallis test. Satisfaction will also be dichotomized and analysed over time with Cochrane-Armitage test for trends.

All instruments used in the study are translationally validated for the country language.

Schedule of Events 9.1.1

Table 1 Study Activities (Day 1/Baseline Through 6 months)

Study Activity

Baselinea Week 12 (V2) ± 7 days

Week 24 (V3) ± 7 days

Early Termination / Drop out

Clin

icia

n Pa

cket

Inclusion/exclusion form X Clinical history/patient demographics X Comorbidities X DAS28 (ESR) or DAS28 (CRP) X X X X

Patie

nt P

acke

t

EuroQoL 5-Dimension (EQ-5D) X X X X Short Form 36-Item Health Survey (SF-36) X X X X Health Assessment Questionnaire (HAQ) X X X X Work Productivity and Activity Impairment Questionnaire (WPAI)

X X X X

Healthcare Resource Utilization (HCRU) X X X X Patient Global Impression of Change (PGIC) X X X Patient Treatment Satisfaction Questions X X X X

Adverse events (including malignancy) X X X X a. The Baseline visit date will serve as the reference for all subsequent visits. A ± 7 day window is

permitted around scheduled study visits.

Setting 9.2

The study will take place in single country (Korea) with multiple centers. The study sites will be identified and selected by AbbVie. The study population shall comprise of male

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and/or female patients who are attending a routine clinical visit and meet all of the inclusion criteria and none of the exclusion criteria. Overall, approximately 89 subjects with clinically diagnosed RA are planned to be enrolled in the study at up to 9 sites. The recruiting investigators will select potentially eligible patients from consecutive visits within their clinic based on the inclusion and exclusion criteria (Section 9.2.1 and Section 9.2.2). It is the responsibility of each physician to ask every consecutive patient who meets the inclusion criteria of the study to participate to avoid selection bias, and if investigators hold different types of clinics (e.g. routine visit clinics versus emergency clinics), only patients visiting their routine clinics will be used for patient selection. Site personnel should thoroughly assess the eligibility criteria and evidence of this should be stored with the source documentation at site. Where there is any deviation from the inclusion/exclusion criteria, the patient should be excluded from the study.

Inclusion Criteria: 9.2.1

Patients meeting all of the following inclusion criteria at baseline will be included: 1. Subject has a diagnosis of RA as defined by the 1987 revised ACR classification

criteria and/or the ACR/ the European League against Rheumatism (EULAR) 2010 classification criteria (any duration since diagnosis)

2. Male or female subjects 18 years of age (local definition according to adalimumab label) who is in compliance with eligibility for adalimumab based on the local label

3. Patients with moderate to severe RA defined as DAS28 (ESR) or DAS28 (CRP)>3.2

4. Biologically treatment naïve and initiated adalimumab at baseline visit 5. Availability of clinical data of the previous 12 weeks prior to baseline 6. Ability to self-complete patient questionnaires 7. Subject must be able and willing to provide written informed consent and comply

with the requirements of this study protocol

Exclusion Criteria: 9.2.2

Patients meeting any of the following exclusion criteria at baseline will be excluded: 1. Patients who are pregnant or breast feeding at enrolment or wish to become

pregnant in the next 24 weeks 2. Participation in any RA-related clinical trial at the time of enrolment, at baseline

or at any point during the past 24 weeks prior to baseline

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3. Patients, who in the clinician’s view, may not be able to accurately report their QoL or prior resource utilization

4. Patients, who in the clinician’s view, may not be able to adhere to adalimumab therapy over 24 weeks

Investigator Selection Criteria 9.2.3

Selection of investigators will be made based on qualification by training and experience. AbbVie will provide IMS with a list of clinicians that would be able to assist in recruiting in a timely manner. IMS will contact each clinician to obtain their participation in the study and provide an expected number of patients to be enrolled from that clinic. The ethical review boards recognized by the respective participating sites are required to review and approve the study and patient informed consent.

Study Procedures 9.2.4

The study procedures outlined in Table 1 will be discussed in detail in this section with the exception of adverse events procedures (discussed in Section11.0). 9.2.4.1 Informed Consent

In local languages will be given to every patient participating in the study before data collection commences. The recruiting clinicians or their representative(s) will provide each patient with the ICF to sign which includes consent to use the data for publication and information including their right to withdraw from the study without penalty or change in medical care the patient is otherwise entitled to.

9.2.4.2 Patient Assignment

Once the recruiting clinician has obtained the subject’s authorization to release medical information and written consent to participate in the study, the clinician will be asked to complete an inclusion and exclusion form (Appendix B) for patients, thus confirming the patient’s eligibility to participate in this study. Each participating patient will be assigned a 3-digit patient identification number. The numbers should be assigned in sequential, ascending order per site as shown below: • Site ID; and

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• Patient ID: First eligible patient number will be 001, and then the second patient number would be 002

X X X X X

Site ID Patient ID

9.2.4.3 Investigator Recruitment

AbbVie will provide IMS with a list of clinicians that would be able to assist in recruiting in a timely manner. IMS will contact each clinician to obtain their participation in the study and provide an expected number of patients to be enrolled from that clinic. The ethical review boards recognized by the respective participating sites are required to review and approve the study and patient informed consent.

9.2.4.4 Study site monitoring

As the study entails patients completing PRO questionnaires and clinicians completing case report forms (CRFs), there is not a need for on-site monitoring visits. IMS will closely track enrolment progress for bi-monthly reporting. IMS will work closely with the study coordinator at each site to ensure they check the forms when returned from the patients and physicians (e.g., all questions were answered). IMS will also be available to answer questions and follow up with the sites if the recruitment process is slow or if there are any errors on the forms. Periodic phone follow-up will be conducted to ensure data collection completeness and quality.

9.2.4.5 Patient Selection

The recruiting investigators will select potentially eligible patients from consecutive visits within their clinic based on the inclusion and exclusion criteria (Section 9.2.1 and Section 9.2.2). It is the responsibility of each physician to ask every consecutive patient who meets the inclusion criteria of the study to participate to avoid selection bias, and if investigators hold different types of clinics (e.g. routine visit clinics versus emergency clinics), only patients visiting their routine clinics will be used for patient selection. The intent is to enroll patients who have been prescribed adalimumab upon the physicians’ own discretion. This study is non-interventional and the subjects/investigator will follow the current clinical practice in each site. Not additional task will be required other than current practice to keep the data as “real world data collect.

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9.2.4.6 Data Collection

IMS will coordinate data collection with each site. At study initiation (Baseline, D0), patients will be asked to provide their written informed consent. The patient then will complete the study questionnaires in paper form. At all follow up visits (week 12 and 24), the patient will complete the study questionnaires while waiting for their appointment at their clinic, approximately 30 minutes before they visit their physicians. It is important that they complete the questionnaires prior to speaking with their clinician during the visit, as the clinician feedback might impact patient perceptions measured by the PRO instruments. Patients must complete the survey by themselves without help from anyone. However, for patients who physically have difficulty filling out the questionnaires, help is allowed as long as there are no suggestions or discussion from the helpers In addition, physicians will also be asked to complete a clinical CRF in paper form based on the patient’s medical records at baseline, 12 weeks, and 24 weeks. The CRF completed by physicians will be returned to the study coordinator/nurse at each site as well. All data filled in by the patient and physician will be collected at each site and returned directly to IMS. The data collection time is expected to be 10-13 months. All patient and clinician data will be handled preserving confidentiality.

9.2.4.7 Study Documents

Clinical case report form (CRF) The clinical CRF will document the patient’s current status (moderate, severe RA), Disease Activity Score in 28 joints (DAS28), prior and current treatments and other relevant clinical and demographic data to be used in segmenting the population during analysis. To calculate the DAS28 the physician or specialist nurse will:

1. Count the number of swollen joints (out of the 28) 2. Count the number of tender joints (out of the 28)

3. Take blood to measure the erythrocyte sedimentation rate (ESR) or C reactive protein (CRP); the latest measurement in the medical records may also be used if a blood draw is not standard for that visit

4. Ask the patient to make a ‘global assessment of health’ which will be indicated by marking a 10 cm line between very good and very bad

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The physician or specialist nurse will then mark each component score on the CRF and the DAS28 score if calculated (an online scoring calculator for the DAS28 can be found at http://www.das-score.nl/das28/DAScalculators/dasculators.html). The DAS28 will be scored using the following formula:

DAS28 ESR = 0.56 * sqrt(tender28) + 0.28 * sqrt(swollen28) + 0.70 * ln(ESR) + 0.014 * (Global assessment of Health in cm)

DAS28 CRP = 0.56 * sqrt(tender28) + 0.28 * sqrt(swollen28) + 0.36 * ln(CRP) + 0.014 * (Global assessment of Health in cm)+0.96

DAS28 scores will be interpreted using the following categorization:

• Remission: DAS28 2.6

• Low Disease activity: 2.6 < DAS28 3.2

• Moderate Disease Activity: 3.2 < DAS28 5.1

• High Disease Activity: DAS28 >5.1

The full CRF is presented in Appendix C. PRO questionnaires The following PRO questionnaires will be included in the patient questionnaire packet. Health Assessment Questionnaire Disability Index (HAQ DI) The HAQ DI is a patient-reported questionnaire to assess functioning impacted by RA. It includes the categories of dressing and grooming, arising, eating, walking, hygiene, reach, grip and common daily activities. It asks patients about the amount of difficulty they experience in these activities as well as the use of aids and/or devices. The HAQ also has a numeric rating scale (NRS) (13) to assess pain on a scale from 0 to 10. Self-administered by the patient, the completion time is approximately 3-4 minutes. The full version of HAQ DI is presented in Appendix D. Short Form (36) Health Survey (SF-36) The SF-36 is a patient-reported questionnaire of patient health-related QoL. It measures generic health concepts relevant across age, disease, and treatment groups. There are 36 items in total and the recall period is the last 4 weeks. The SF-36 consists of eight scaled scores, which are the weighted sums of the questions in their section. Each scale is directly transformed into a 0-100 scale. Completion time for the SF-36 is approximately 10 minutes. The full version of SF-36 is presented in Appendix E.

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EuroQol 5 dimension, 3 level quality of life questionnaire (EQ-5D-3L) The EQ-5D-3L measures the patient’s overall health state in a descriptive system of health-related QoL states consisting of five dimensions (mobility, self-care, usual activities, pain/discomfort, and anxiety/depression) each of which can take one of three responses. The responses record three levels of severity (‘no problems’, ‘some problems’, and ‘extreme problems) within a particular EQ-5D-3L dimension (14,15). In addition, a VAS rates current health state between 0-100. The EQ-5D-3L results can be converted to health utility scores. Completion time for the EQ-5D-3L is approximately 2-3 minutes. The full version of EQ-5D-3L is presented in Appendix F. Work Productivity and Activity Impairment (WPAI) The WPAI is a patient-reported questionnaire to measure work and activity impairment during the past seven days. It determines employment status, hours missed from work due to the disease (i.e. RA), hours missed from work for other reasons, hours actually worked, the degree to which the disease affected work productivity while at work and the degree to which the disease affected activities outside of work. Additional questions around employment status will be incorporated into the survey. The completion time for the WPAI is approximately 2-5 minutes. The full version of WPAI is presented in Appendix G. Patient Global Impression of Change (PGIC) The PGIC measures the patient’s perceptions of changes in their disease. It consists of one question asking about the change in their condition; for this study, the base will be “since you initiated your adalimumab treatment”. The completion time for the PGIC is less than 1 minute. The full version of PGIC is presented in Appendix H. Patient Treatment Satisfaction Questions The patient treatment satisfaction questions were developed de novo for this study and are not considered “validated” questions. Self-administered by the patient, the completion time for the patient treatment satisfaction questions is approximately 1-2 minutes. The full version of patient treatment satisfaction questions are presented in Appendix I. Healthcare Resource Utilization (HCRU) Questionnaire The HCRU questionnaire will collect data on the healthcare resources consumed in the prior 3 months, as recall beyond 3 months may be problematic in an older population(16). HCRU collection will include data such as the number of physician visits and to which physician (GP, specialist), Emergency Department visits, hospitalizations, and other drugs

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as well as devices and aids purchased to assist in their mobility due to RA. The HCRU questionnaire will be part of the patient questionnaire and will be distributed to patients together with the PRO questionnaires (Appendix D to Appendix I). The full HCRU questionnaire is presented in Appendix J. All of the questionnaires will use the validated Korean version.

Adverse Events 9.2.5

Adverse events, whether in response to a query, observed by site personnel, or reported spontaneously by the subject will be recorded. Adverse events definition and serious adverse event categories are described in detail in Section 11.0.

Variables 9.3

Variables: Primary Variable

Change in HAQ DI score at weeks 12 and weeks 24 weeks from the baseline Secondary Variable

Change in other PROs (SF-36 domain scales, EQ-5D Index, Work Productivity and Activity Impairment Questionnaire [WPAI]) from baseline to weeks 12 and 24

Change in patient satisfaction questions from baseline to weeks 12 and 24

Number and percent of patients achieving a clinically meaningful improvement on the HAQ DI, from baseline to weeks 12 and 24

Healthcare Resource Utilization (HCRU) at baseline, 12 and 24 weeks

Additional Secondary Variable Change in HAQ DI score from baseline to 24 weeks Changes in the disease severity and PROs from baseline to 24 weeks

Data Sources 9.4

Case Report Forms (CRFs) and patient questionnaires.

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Collection of data includes but not limited to subject demographics, clinical history, comorbidities, spontaneous adverse events, and concomitant medications. The following questionnaires will be utilized to collect data directly from participating subjects:

EQ-5D SF-36 HAQ DI WPAI HCRU Patient Global Impression of Change (PGIC) Patient Treatment Satisfaction Questions

Study Size 9.5

Approximately 89 patients diagnosed with RA will be recruited. The sample size was calculated by assuming an alpha of 0.05 and a power of 0.80 in a one-sided test, Z (1-alpha) = 1.645 and Z (1-β) = 0.842. As to the primary variable, assuming a mean ΔHAQ-DI of -0.21 and a standard deviation (SD) of 0.5, according to the formula, 36 subjects are required. Then, given the importance of the secondary endpoint (WPAI), an improvement of 9.9±25 hours of work time lost (mean=9.9, SD=25) requires 40 subjects. However, we assume a 50% employment rate in the study population and a drop-out rate of 10%, eventually approximately 89 patients will be required (40/0.5/(1-0.1) = 89).

Data Management and Storage Process 9.6

Data Management 9.6.1

Data management and data quality check will be performed to remove errors and inconsistencies in order to assure the appropriateness of the study data set to assess the study objectives. Data entry screens will be developed and tested prior to initiating data collection to reduce data entry errors. If required, IMS will provide AbbVie with data for analysis. Each principle investigator or his/her designees will be instructed to answer patients’ queries which may arise in relation to the questionnaires and check the patients’ input to make sure all questions are answered.

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Storage Process 9.6.2

Following data quality checks, each dataset will be converted to SAS and merged for analysis. All information included in the CRF and the patients’ questionnaires will be checked in order to detect possible queries to solve and will be extracted to a specifically designed database, where it will be validated by IMS personnel to ensure its quality. Finally, data analysis will be conducted and final results reported. The databases will be stored in IMS data servers. Data servers are submitted to daily backups in order to increase the security on all data managed in the collection process. All paper based questionnaires will be stored in a secured, locked area for a period of seven (7) years, after which all data will be shared using an agency specialized in disposal of confidential documents.

Data Analysis 9.7

Statistical and Analytic plans 9.7.1

A statistical analysis plan (SAP) will be developed describing the specific analysis that will be performed including, and in addition to, the analysis described here. All analysiswill be performed in accordance with the approved analysis plan. The following provides an overview of some of the analysis. The scoring of the PRO questionnaires will be done in accordance to the developers’ recommendations. A separate statistical analysis plan will be developed describing the specific analysis that will be performed including and in addition to the analysis described here.

Analyzable population 9.7.2

All subjects who received at least one dose of adalimumab during the study will be included. The main analysis will be conducted on the pooled population, where appropriate, with each individual country analyzed separately as supportive data.

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Planned Methods of Statistical Analysis 9.7.3

All statistical tests will be two-tailed with a significance level of 0.05. Descriptive statistics will be provided. Descriptive analysis will be conducted on all key parameters and presented as mean, standard deviation, minimum, maximum, and median when continuous and as “n” and percent when categorical. Change from adalimumab initiation to 24 weeks will be calculated and evaluated for significant improvements using paired t-tests / ANOVA for parametric and Wilcoxon signed-rank for non-parametric data. Analysis will be also be conducted by severity level (moderate vs severe), disease duration quartile (to compare to prior work) and up to two (2) other subgroups. Cochran-Armitage test of trends or other similar methods may be used to compare categories of subjects.

Primary Endpoint Analysis 9.7.4

The primary endpoint variable will be the change in HAQ DI score at 24 weeks after the initiation of adalimumab (observed population). The objective of the primary endpoint analysis will be to demonstrate that treatment with adalimumab improves functioning as measured by the HAQ DI in subjects with RA following treatment initiation. This change will be summarized as the mean and 95% confidence interval and will be tested with a paired t-test. The primary analysis will be summarized as the mean and 95% confidence interval and will be tested with a paired t-test without adjusting for baseline disease severity. For sensitivity analysis, the mean change in HAQ DI at Week 24 will be analyzed using ANOVA adjusting for baseline disease severity.

Secondary Endpoint Analysis 9.7.5

The main secondary endpoint variable will be the change in HAQ DI at 12 weeks after the initiation of adalimumab. The objective of endpoint analysis will be to demonstrate that treatment with adalimumab improves functioning as measured by HAQ DI in subjects with RA compared to baseline. The main secondary analysis will be summarized as the mean and 95% confidence interval and will be tested with a paired t-test without adjusting for baseline disease severity. For sensitivity analysis, the mean change in HAQ DI at Week 12 will be analyzed using ANOVA adjusting for baseline disease severity.

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Other secondary analysis include:

Change in other patient reported outcomes (SF-36 domain scales, EQ-5D Index, WPAI total lost productivity) at weeks 12 and 24 after the initiation of adalimumab, in those patients continuing on adalimumab (observed population). These changes will be summarized as the means and 95% confidence intervals and will be tested with paired t-tests.

Number and percent of patients achieving a clinically meaningful improvement on the HAQ DI, as defined by a -0.22 point improvement or greater, at weeks 12 and 24 after the initiation of adalimumab (observed population).

Additional Secondary Endpoint Analysis 9.7.6

Additional efficacy analysis includes: Change in HAQ DI score at 24 weeks after the initiation of adalimumab, in those

patients continuing on adalimumab, compared with those patients not continuing on adalimumab. The mean changes in these two groups will be compared using an independent t-test.

Healthcare resource utilization will be described using number and percentage within each category (number of consultations, number of procedures received, number of surgeries, number of hospitalizations and length of stay, number of concomitant medications)

Associations between disease severity and PROs Associations between change in disease severity and change in PROs

Exploratory endpoint Change in patient satisfaction questions at weeks 12 and 24 after the initiation of adalimumab (observed population). These changes will be summarized as number and percentage of each response and compared with Kruskal–Wallis test. Satisfaction will also be dichotomized and analyzed over time with Cochrane-Armitage test for trends.

Safety Analysis 9.7.7

Adverse events occurring while participants are on adalimumab will be coded using Common Terminology Criteria for Adverse Events (CTCAE) classification individually listed by indication groups. The incidences and percentages of individuals experiencing AEs and SAEs within each indication will be summarized by System Organ Class (SOC) with further summaries by severity and relatedness (causality) categories. Adverse events

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leading to discontinuation and concomitant medications will also be listed and summarized.

Additional Analysis 9.7.8

Additional analysis will explore the potential modifying effects of baseline measures on the changes in primary and secondary efficacy outcomes. These measures will include age, gender, baseline severity, and other diagnoses/co-morbidities. The analysis will specifically test for differential changes across the subgroups defined by the potential modifiers using general linear models.

Missing Data 9.7.9

Efficacy measures are not assessed after a participant discontinues adalimumab. The exception to this will be the analysis of proportion of patients at 24 weeks who remain on adalimumab. Item level data on the PROs will be imputed according to the developers’ recommendations. There will be no other imputation for missing data.

Interim Analysis 9.7.10

There is no interim analysis planned for this study.

Quality Control 9.8

Ethics and Quality 9.8.1

Prior to any study-related data being collected, informed consent form will be reviewed, signed and dated by the patient and the person who administered the informed consent. A copy of the signed informed consent will be given to the patient and the original will be placed in the patient's medical record.

Quality Assurance 9.8.2

Prior to the initiation of the study, physician and site personnel will be trained on the study. Training will include a detailed discussion of the protocol, performance of study procedures, and completion of the CRFs and paper questionnaires.

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All sites will be monitored during the course of study participation. One hundred percent (100%) source document review for safety will be performed. All clinical data will be documented via the CRF. Study coordinators at each site will check the paper CRFs completed by the physicians and questionnaires completed by patients (e.g., all questions were answered). Data entry will be conducted by IMS. After entry of the data, computer logic checks will be run to check for inconsistent data. Any necessary corrections will be made to the database and documented via addenda, queries, and source data clarification forms. Steps to be taken to ensure the accuracy and reliability of data include the selection of qualified investigators and appropriate study centers, review of protocol procedures with the investigator and associated personnel before the study and periodic monitoring visits by the sponsor. Written instructions will be provided for administration and collection of study questionnaires. Guidelines for CRF completion will be provided and reviewed with study personnel before the start of the study. The sponsor will review CRFs and patient questionnaires for accuracy and completeness after transmission to the sponsor; any discrepancies will be resolved with the investigator or designee, as appropriate. After upload of the data into the clinical study database they will be verified for accuracy and consistency with the data sources.

Limitations of the Research Methods 9.9

The study is to be performed as a non-interventional study. Unlike clinical studies, obtainable data are limited and there is a possibility of missing data.

Other Aspects 9.10

Note to File 9.10.1

The Principal Investigator or designee will be responsible for documenting study relevant information and occurrences that affects the course of the study. The information and occurrences are not protocol deviations but will be documented in a note to file and will be communicated to the sponsor.

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Training Log 9.10.2

All designated study personnel must be trained on the study protocol and procedures. Training and retraining are documented on the Training Log.

Visitor Log 9.10.3

All Sponsor or other related individuals who visit the study site must sign the Visitor Log.

Responsibilities of the Principal Investigator 9.10.4

The Principal Investigator is responsible for oversight of enrolment, the patient consent process, study related procedures, compliance with the protocol, all institutional, state and local guidelines. It is the responsibility of the Principal Investigator to select, supervise, and delegate responsibility for study conduct to staff members. The Principal Investigator is responsible for determining the appropriate staff qualifications required for specific study-related tasks to be delegated. Study-related tasks delegated to staff members will be documented on the Site Signature and Delegation Log.

End of Trial 9.10.5

End of Trial is defined as last subject’s last visit (LSLV).

10.0 Protection of Human Subjects

This study must be conducted in compliance with the recommendations of the Declaration of Helsinki, 2008 (World Medical Association). In addition, this study will adhere to all general and local legal and regulatory requirements applicable to non-interventional studies. Informed consent will be obtained from each subject before the subject can participate in the study. The contents and process of obtaining informed consent will be in accordance with all applicable regulatory requirements.

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As required by applicable local regulations, the sponsor’s Regulatory Affairs group will ensure all legal regulatory aspects are covered, and obtain approval of the appropriate regulatory bodies, prior to study initiation in regions where an approval is required. This study is non-interventional and falls outside the scope of the EU Directive 2001/20/EC, the EU Directive 2005/28/EC and International Conference on Harmonization (ICH) Good Clinical Practice (GCP) guidelines. This study complies with the EU Directive 95/46/EC of the European Parliament and of the Council of 24 October 1995 on the protection of individuals with regard to the processing of personal data and on the free movement of such data.

11.0 Management and Reporting of Complaints

A Complaint is any written, electronic, or oral communication that alleges deficiencies related to the physical characteristics, identity, quality, purity, potency, durability, reliability, safety, effectiveness, or performance of a product/device after it is released for distribution.

The investigational product in this trial contains both:

● Biologic compound(s) and ● Device component(s) (pre-filled syringe, pen).

Complaints associated with any component of this investigational product must be reported to the Sponsor (Section 11.2.2). For adverse events, please refer to Sections 11.1.1 through11.1.6. For product complaints, please refer to Section 11.2

Medical Complaints 11.1

Adverse Event Definition and Serious Adverse Event Categories 11.1.1

An adverse event (AE) is defined as any untoward medical occurrence in a patient, which does not necessarily have a causal relationship with their treatment. An adverse event can therefore be any unfavorable and unintended sign (including an abnormal laboratory finding), symptom, or disease temporally associated with the use of a medicinal product, whether or not the event is considered causally related to the use of the product.

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Such an event can result from use of the drug as stipulated in the labeling, as well as from accidental or intentional overdose, drug abuse, or drug withdrawal. Any worsening of a pre-existing condition or illness is considered an adverse event. If an adverse event meets any of the following criteria, it is considered a serious adverse event (SAE):

Death of Patient: An event that results in the death of a patient.

Life-Threatening: An event that, in the opinion of the investigator, would have resulted in immediate fatality if medical intervention had not been taken. This does not include an event that would have been fatal if it had occurred in a more severe form.

Hospitalization: An event that results in an admission to the hospital for any length of time. This does not include an emergency room visit or admission to an outpatient facility.

Prolongation of Hospitalization:

An event that occurs while the study patient is hospitalized and prolongs the patient's hospital stay.

Congenital Anomaly: An anomaly detected at or after birth, or any anomaly that results in fetal loss.

Persistent or Significant Disability/Incapacity:

An event that results in a condition that substantially interferes with the activities of daily living of a study patient. Disability is not intended to include experiences of relatively minor medical significance such as headache, nausea, vomiting, diarrhea, influenza, and accidental trauma (e.g., sprained ankle).

Important Medical Event Requiring Medical or Surgical Intervention to Prevent Serious Outcome:

An important medical event that may not be immediately life-threatening or result in death or hospitalization, but based on medical judgment may jeopardize the patient and may require medical or surgical intervention to prevent any of the outcomes listed above (i.e., death of patient, life threatening, hospitalization, prolongation of hospitalization, congenital anomaly, or persistent or significant

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disability/incapacity). Additionally, any elective or spontaneous abortion or stillbirth is considered an important medical event. Examples of such events include allergic bronchospasm requiring intensive treatment in an emergency room or at home, blood dyscrasias or convulsions that do not result in inpatient hospitalization, or the development of drug dependency or drug abuse.

Severity 11.1.2

The following definitions will be used to rate the severity for any adverse event being collected as an endpoint/data point in the study and for all serious adverse events.

Mild: The adverse event is transient and easily tolerated by the patient.

Moderate: The adverse event causes the patient discomfort and interrupts the patient's usual activities.

Severe: The adverse event causes considerable interference with the patient's usual activities and may be incapacitating or life threatening.

Relationship to Pharmaceutical Product 11.1.3

The following definitions will be used to assess the relationship of the adverse event to the use of product:

Reasonable Possibility An adverse event where there is evidence to suggest a causal relationship between the product and the adverse event.

No Reasonable Possibility An adverse event where there is no evidence to suggest a causal relationship between the product and the adverse event.

If no reasonable possibility of being related to product is given, an alternate etiology must be provided for the adverse event.

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Serious Adverse Event Collection Period 11.1.4

Serious adverse events will be reported to AbbVie from the time the physician obtains the patient's authorization to use and disclose information (or the patient's informed consent) until 30 days or 5 half-lives following the intake of the last dose of physician-prescribed treatment.

Serious Adverse Event Reporting 11.1.5

In the event of a serious adverse event, the physician will: For events from patients using and AbbVie product - notify the AbbVie

contact person identified below within 24 hours of the physician becoming aware of the event.

Pregnancy Reporting 11.1.6

In the event of a pregnancy occurrence in the patient, the physician will notify AbbVie contact person identified in Section 11.1.5 within 24 hours of the physician becoming aware of the pregnancy.

Malignancy Reporting 11.1.7

In the event of any non-serious event of malignancy in subjects 30 years of age and younger, whether related to adalimumab or not, the investigator will notify AbbVie Emergency contact person identified at the beginning of the protocol within 24 hours of the site being made aware of the event. Adalimumab therapy has a well-established and well described safety profile based on extensive postmarketing experience and continued clinical trial patient exposure since the first approved indication in 2002 for rheumatoid arthritis. A detailed discussion of the pre-clinical toxicology, metabolism, pharmacology and safety experience with adalimumab can be found in the current Investigator's Brochure. AbbVie is committed to continue to collect safety information including those events that may occur in this trial in order to

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confirm this established safety profile and to identify any unknown potential adverse reactions, rare events and those events with a long latency. AbbVie is participating in an FDA-requested, TNF inhibitor class wide exploration of the rare appearance of malignancy in subjects/patients who are 30 years of age or younger at the time of diagnosis. The risk of malignancy in this age group has not been established and is difficult to study due to its rarity. AbbVie appreciates your attention to the additional reporting requirements needed in this unlikely event, outlined in Section 11.7 under Malignancy Reporting.

Product Complaint 11.2

Definition 11.2.1

A Product Complaint is any Complaint (see Section 11.0 for the definition) related to the biologic or drug component of the product or to the medical device component(s).

For a product this may include, but is not limited to, damaged/broken product or packaging, product appearance whose color/markings do not match the labeling, labeling discrepancies/inadequacies in the labeling/instructions (example: printing illegible), missing components/product, device not working properly, or packaging issues.

For medical devices, a product complaint also includes all deaths of a patient using the device, any illness, injury, or adverse event in the proximity of the device, an adverse event that could be a result of using the device, any event needing medical or surgical intervention including hospitalization while using the device and use errors.

Any information available to help in the determination of causality by the device to the events outlined directly above should be captured.

Reporting 11.2.2

Product Complaints concerning the investigational product and/or device must be reported to the Sponsor within 24 hours of the study site's knowledge of the event via local Product Complaint reporting practices. Product Complaints occurring during the study will be followed-up to a satisfactory conclusion. All follow-up information is to be reported to the Sponsor (or an authorized representative) and documented in source as required by the

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Sponsor. Product Complaints associated with adverse events will be reported in the study summary. All other complaints will be monitored on an ongoing basis.

Product complaints involving a non-Sponsor investigational product and/or device should be reported to the identified contact or manufacturer, as necessary per local regulations.

Product Complaints may require return of the product with the alleged complaint condition (syringe, pen, etc.). In instances where a return is requested, every effort should be made by the investigator to return the product within 30 days. If returns cannot be accommodated within 30 days, the site will need to provide justification and an estimated date of return.

The description of the complaint is important for AbbVie in order to enable AbbVie to investigate and determine if any corrective actions are required.

12.0 Ethical and Legal Consideration

All participant data will be handled in a manner compliant with all local regulatory and privacy laws. All parties will ensure protection of subject personal data and will not include subject names on any sponsor forms, reports, publications, or in any other disclosures, except where required by law. Appropriate role-based access to minimum necessary information will be maintained so that only authorized individuals have access to protected health information (PHI). Abbvie shall comply with all applicable laws regarding the reporting of spontaneous adverse events (AEs) to the relevant local authorities in Korea. Abbvie will follow the International Conference on Harmonization of Good Clinical Practice (ICH-GCP) guidelines for AE reporting and report all spontaneously reported AEs within the required timeframe (usually within 24 hours of discovery). All IMS staff working directly with patient data and/or having direct contact with healthcare practitioners will have received formal training to ensure they have a clear understanding of how to recognize an AE and inform Affiliate Safety Specialist so that they are in full compliance with local laws regarding AE reporting.

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The study will be reviewed and approved by the appropriate Ethics Committee(s) at each site prior to the start of patient recruitment, according to the specific legal requirements in each country.

13.0 Confidentiality

Patient confidentiality 13.1

Information on patients’ identity shall be considered as confidential for all effects and purposes. Each site and patient will have a code in the study. Sites will be automatically coded by IMS. Patients will be assigned a sequential number by the site coordinator upon meeting all inclusion and no exclusion criteria. The patients’ identity should not be revealed nor published under any circumstances. Patient data recorded in the CRF will be documented anonymously, coded with a patient number in such a way that only the investigator and site staff may associate particular data with an identified or identifiable individual or his/her medical record. All other parties involved in data management, analysis and storage will receive, and subsequently analyze, non-identifiable patient data.

Data confidentiality 13.2

By signing the investigator’s confidentiality agreement, the investigator affirms to AbbVie/IMS that information furnished by AbbVie/IMS to the investigator will be kept in confidence and such information will be divulged to any expert committee, affiliated institution, and employees only under an appropriate understanding of confidentiality with such committee, affiliated institution and employees.

14.0 Study administration

The entire study will be managed by an international project coordinator at IMS Japan K.K. who will coordinate the project and maintain fluid communication with the study sponsor, the study team and the director at IMS Japan K.K. As part of the monitoring plan, regular phone calls (at least every two weeks) will be made between IMS and local site coordinator in order to check inclusion status, resolve any issues, check data plausibility, etc.

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15.0 Investigators compliance

By signing the investigator’s agreement, the investigator agrees to conduct the study in an efficient and diligent manner and in conformance with this protocol, generally accepted standards of good clinical practice and all applicable laws, rules and regulations relating to the conduct of the study. The investigator shall prepare and maintain complete and accurate study documentation in compliance with applicable national and local laws, rules and regulations and, for each patient participating in the study, promptly record all data in the CRF as required by this protocol.

16.0 Risks

This is a non-interventional observational study. It does not involve any direct patient intervention with respect to laboratory tests, examinations or drug treatment. Patients will be asked to complete questionnaires related to their RA, QoL, functioning, work productivity, treatment satisfaction, and healthcare resource utilization at their clinic during their visit three times over the course of 6 months, requiring approximately 30 minutes of their time each time.

17.0 Discontinuation or Drop-out

Patients’ participation in the study is completely voluntary, and they are allowed to withdraw or discontinue from the study. The following three situations will be counted as study drop-out:

1) Patient is switched off Adalimumab 2) Patient is not willing to continue participation in the study 3) Patient disappears and cannot be contacted anymore

For the first two situations, the Early Termination Form (Appendix K) will be provided for the patients and their physicians to fill in. Patients not completing questionnaires will not be classified as drop-out. For example, if a patient missed Week 12 questionnaires for some reason, he/she can still fill in Week 24 questionnaires.

Once a subject is dropped out from the study, no further information for that subject will be collected. However, the reason for drop-out will be collected and, if the reason for treatment discontinuation is due to as adverse event, the event will be reported as follows :

SAE : reported to Abbvie within 24 hours of physician awareness

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Non-serious AE : reported to Abbvie within 24 hours of PMOS physician awareness.

18.0 Quality control and audit

Steps to be taken to ensure the accuracy and reliability of data include the selection of qualified investigators and appropriate study centers, review of protocol procedures with the investigator and associated personnel before the study and periodic monitoring visits by the sponsor. Written instructions will be provided for administration and collection of study questionnaires. Guidelines for CRF completion will be provided and reviewed with study personnel before the start of the study. The sponsor will review CRFs and patient questionnaires for accuracy and completeness during on-site monitoring visits and after transmission to the sponsor; any discrepancies will be resolved with the investigator or designee, as appropriate. After upload of the data into the clinical study database they will be verified for accuracy and consistency with the data sources. The study will be performed following the IMS and AbbVie Standard Operating Procedures (SOPs) for Observational Studies.

19.0 Communication of findings

AbbVie / IMS shall retain ownership of all screeners, case report forms, data analysis, and reports which result from this study. All information obtained as a result of the study will be regarded as confidential, until appropriate analysis and review by AbbVie and the investigator(s) are completed. The results of the study may be published or presented by the investigator(s) after the review by, and in consultation and agreement with AbbVie, such that confidential or proprietary information is not disclosed. Prior to publication or presentation, a copy of the final text should be forwarded by the investigator(s) to AbbVie for comment. Such comments shall aim to ensure the scientific content of the proposed publications and/or presentations and ensure that the data and material receive fair, accurate, and reasonable presentation.

20.0 References

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1 World Healht Organisation. Disability Fact Sheet. [cited May 7, 2015]; Available from: http://www.who.int/disabilities/world_report/2011/factsheet.pdf

2 AbbVie Limited. Adalimumab Data Sheet. 27 November 2014(Version 32). 3 U.S. Department of Health and Human Services, Food and Drug Administration, Center

for Drug Evaluation and Research (CDER), Center for Biologics Evaluation and Research (CBER), (CDRH) CfDaRH. Guidance for Industry Rheumatoid Arthritis: Developing Drug Products for Treatment. 2013.

4 Bruce B, Fries J. The health assessment questionnaire (HAQ). Clinical and experimental rheumatology. 2005;23(5):S14.

5 Bruce B, Fries JF. The Stanford Health Assessment Questionnaire: a review of its history, issues, progress, and documentation. The Journal of rheumatology. 2003;30(1):167-78.

6 Barrett EM, Scott DG, Wiles NJ, Symmons DP. The impact of rheumatoid arthritis on employment status in the early years of disease: a UK community-based study. Rheumatology (Oxford, England). 2000 Dec;39(12):1403-9.

7 Wolfe F, Hawley DJ. The longterm outcomes of rheumatoid arthritis: Work disability: a prospective 18 year study of 823 patients. The Journal of rheumatology. 1998 Nov;25(11):2108-17.

8 Jantti J, Aho K, Kaarela K, Kautiainen H. Work disability in an inception cohort of patients with seropositive rheumatoid arthritis: a 20 year study. Rheumatology (Oxford, England). 1999 Nov;38(11):1138-41.

9 Fex E, Larsson BM, Nived K, Eberhardt K. Effect of rheumatoid arthritis on work status and social and leisure time activities in patients followed 8 years from onset. The Journal of rheumatology. 1998 Jan;25(1):44-50.

10 Dougados M, Schmidely N, Le Bars M, et al. Evaluation of different methods used to assess disease activity in rheumatoid arthritis: analysis of abatacept clinical trial data. Annals of the rheumatic diseases. 2009 Apr;68(4):484-9.

11 van der Bijl AE, Breedveld FC, Antoni CE, et al. An open-label pilot study of the effectiveness of adalimumab in patients with rheumatoid arthritis and previous infliximab treatment: relationship to reasons for failure and anti-infliximab antibody status. Clinical rheumatology. 2008 Aug;27(8):1021-8.

12 Bejarano V, Quinn M, Conaghan PG, et al. Effect of the early use of the anti-tumor necrosis factor adalimumab on the prevention of job loss in patients with early rheumatoid arthritis. Arthritis and rheumatism. 2008 Oct 15;59(10):1467-74.

13 Hawker GA, Mian S, Kendzerska T, French M. Measures of adult pain: Visual Analog Scale for Pain (VAS Pain), Numeric Rating Scale for Pain (NRS Pain), McGill Pain Questionnaire (MPQ), Short-Form McGill Pain Questionnaire (SF-MPQ), Chronic Pain Grade Scale (CPGS), Short Form-36 Bodily Pain Scale (SF-36 BPS), and Measure of Intermittent and Constant Osteoarthritis Pain (ICOAP). Arthritis care & research. 2011 Nov;63 Suppl 11:S240-52.

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14 The EuroQol Group. EuroQol--a new facility for the measurement of health-related quality of life. Health policy (Amsterdam, Netherlands). 1990 Dec;16(3):199-208.

15 Oemar M, Oppe M. EQ-5D-3L User Guide: Basic information on how to use the EQ-5D-3L instrument. The EuroQol Group; 2013.

16 Evans C, Crawford B. Patient self-reports in pharmacoeconomic studies. Their use and impact on study validity. PharmacoEconomics. 1999 Mar;15(3):241-56.

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21.0 Appedndices

Appendix A. Patient Informed Consent Form (ICF)

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Appendix B. Inclusion/Exclusion Form

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Appendix C. Clinical Case Report Form (CRF) Baseline:

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Follow-up:

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Appendix D. Health Assessment Questionnaire Disability Index (HAQ DI)

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Appendix E. Short Form (36) Health Survey (SF-36)

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Appendix F. EuroQol 5 dimension, 3 level quality of life questionnaire (EQ-5D-3L)

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Appendix G. Work Productivity and Activity Impairment (WPAI)

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Appendix H. Patient Global Impression of Change (PGIC)

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Appendix I. Patient Treatment Satisfaction Questions

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Appendix J. Healthcare resource utilization (HCRU) questionnaire Baseline:

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Follow-up:

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Appendix K. Early Termination FormFor Physician:

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For Patient:

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Appendix L. Amendment 01 Changes Summary of Amendment changes:

• Change of sample size • Change of milestones

Section 4.0 Abstract Previously read:

Study Design RA patients, for whom adalimumab treatment has already been decided, will be recruited from within the clinical settings of each rheumatologist participating in the study. Approximately 100 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea.

Population Subjects will be males and/or females who are attending a routine clinical visit and meet all of the inclusion criteria and none of the exclusion criteria. Approximately 100 patients diagnosed with RA will be recruited.

Study Size Approximately 100 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea. The sample size was calculated by assuming an alpha of 0.05 and a power of 0.80 in a two-sided test, resulting in 52 subjects required to recognize a statistically significant improvement in HAQ DI (-0.21). Given the importance of other secondary endpoints, an improvement of 9.9±25 hours of work time lost requires 58 subjects, assuming an alpha of 0.05 and a power of 0.80 in a two-sided test. However, since it is expected that approximately half the study population may no longer be working due to their age, approximately twice this number (100 patients) will be required to achieve the required number of respondents. We have also assumed a drop-out rate of 13% (assuming between 10%-15%).

Milestones Start of Data Collection: 19 Oct, 2015 End of Data Collection: 31 Jan, 2017 Study Progress Report: Not applicable Interim Report: Not applicable

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Registration in the EU PASS Register: Not Applicable Final Report of Study Results: 31 Jul, 2017 Has been changed to read:

Study Design RA patients, for whom adalimumab treatment has already been decided, will be recruited from within the clinical settings of each rheumatologist participating in the study. Approximately 89 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea.

Population Subjects will be males and/or females who are attending a routine clinical visit and meet all of the inclusion criteria and none of the exclusion criteria. Approximately 89 patients diagnosed with RA will be recruited.

Study Size Approximately 89 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea. The sample size was calculated by assuming an alpha of 0.05 and a power of 0.80 in a one-sided test, resulting in 36 subjects required to recognize a statistically significant improvement in HAQ DI (-0.21). Then, given the importance of other secondary endpoints, an improvement of 9.9±25 hours of work time lost requires 40 subjects. However, since it is expected that approximately half the study population may no longer be working due to their age, we assume a 50% employment rate in the study population and a drop-out rate of 10%, eventually approximately 89 patients will be required to achieve the required number of respondents.

Milestones Start of Data Collection: 19 Oct, 2015 End of Data Collection: 28 Feb, 2018 Study Progress Report: Not applicable Interim Report: Not applicable Registration in the EU PASS Register: Not Applicable Final Report of Study Results: 31 Aug, 2018

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Section 6.0 Milestones Previously read: Major study milestones and their planned dates are as follows: Start of Data Collection (FPFV): 19 October 2015 End of Data Collection: 31 January 2017 Study Progress Report: Not Applicable Interim Report: Not Applicable Registration in the EU PAS register: Not Applicable Final Report of Study Results: 31 July 2017 Has been changed to read: Major study milestones and their planned dates are as follows: Start of Data Collection (FPFV): 19 October 2015 End of Data Collection: 28 February 2018 Study Progress Report: Not Applicable Interim Report: Not Applicable Registration in the EU PAS register: Not Applicable Final Report of Study Results: 31 August 2018 Section 9.1 Study Design Previously read: Approximately 100 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea. Has been changed to read: Approximately 89 patients diagnosed with RA that meet the inclusion and exclusion criteria will be enrolled at approximately 9 sites in Korea.

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Section 9.2 Setting Previously read: Overall, approximately 100 subjects with clinically diagnosed RA are planned to be enrolled in the study at up to 9 sites. Has been changed to read: Overall, approximately 89 subjects with clinically diagnosed RA are planned to be enrolled in the study at up to 9 sites. Section 9.5 Study Size Previously read: Approximately 100 patients diagnosed with RA will be recruited. The planned sample size provides at least 95% power for detecting a statistically significant improvement in HAQ-DI (∆HAQ-DI < 0) assuming a mean ∆HAQ-DI of -0.21 and a standard deviation of 0.5 (reference 11), at two-sided significance level of 0.05 and accounting for a 10% dropout rate. The sample size also provides at least 95% power for detecting a statistically significant clinically meaningful improvement in HAQ-DI (∆HAQ-DI < -0.22) assuming a mean ∆HAQ-DI of -0.5 and a standard deviation of 0.7, at two-sided significance level of 0.05 and accounting for a 10% dropout rate. For the secondary endpoint WPAI, the sample size provides 63% power for detecting a statistically significant improvement in “hours of work lost” at two-sided significance level of 0.05 and accounting for a 10% dropout rate, assuming a mean change in “hours of work lost” of 10 and standard deviation of 30 and assuming a 55% employment rate in the study population. Has been changed to read: Approximately 89 patients diagnosed with RA will be recruited. The sample size was calculated by assuming an alpha of 0.05 and a power of 0.80 in a one-sided test, Z (1-alpha) = 1.645 and Z (1-β) = 0.842. As to the primary variable, assuming a mean ΔHAQ-DI of -0.21 and a standard deviation (SD) of 0.5, according to the formula, 36 subjects are required. Then, given the importance of the secondary endpoint (WPAI), an improvement of 9.9±25 hours of work time lost (mean=9.9, SD=25) requires 40 subjects. However, we assume a 50% employment rate in the study population and a drop-out rate of 10%, eventually approximately 89 patients will be required (40/0.5/(1-0.1) = 89).

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